Glyme-Li salt equimolar molten solvates with iodide/triiodide redox anions.

Room-temperature-fused Li salt solvates that exhibit ionic liquid-like behaviour can be formed using particular combinations of multidentate glymes and lithium salts bearing weakly coordinating anions, and are now deemed a subset of ionic liquids, viz. solvate ionic liquids (SILs). Herein, we report redox-active glyme-Li salt molten solvates consisting of tetraethyleneglycol ethylmethyl ether (G4Et) and lithium iodide/triiodide, [Li(G4Et)]I and [Li(G4Et)]I3. The coordination structure of the complex ions and the thermal, transport, and electrochemical properties of these molten Li salt solvates were investigated to diagnose whether they can be categorized as SILs. [Li(G4Et)]+ and I3 - were found to remain stable as discrete ions and exist as well-dissociated forms in the liquid state, indicating that [Li(G4Et)]I3 can be classified as a good SIL. This study also clarified that the I- and I3 - counter anions exhibit an electrochemical redox reaction in the highly concentrated molten Li salt solvates. The redox-active molten Li solvates were further studied as a highly concentrated catholyte for use in rechargeable semi-liquid lithium batteries. Although the cell constructed using [Li(G4Et)]I3 failed to charge after the initial discharge step, the cell containing [Li(G4Et)]I demonstrates reversible charge-discharge behaviour with a high volumetric energy density of 180 W h L-1 based on the catholyte volume.

Stability of Glyme Solvate Ionic Liquid as an Electrolyte for Rechargeable Li-O2 Batteries.

A solvate ionic liquid (SIL) was compared with a conventional organic solvent for the electrolyte of the Li-O2 battery. An equimolar mixture of triglyme (G3) and lithium bis(trifluoromethanesulfonyl)amide (Li[TFSA]), and a G3/Li[TFSA] mixture containing excess glyme were chosen as the SIL and the conventional electrolyte, respectively. Charge behavior and accompanying gas evolution of the two electrolytes was investigated by electrochemical mass spectrometry (ECMS). From the linear sweep voltammetry performed on an as-prepared cell, we demonstrate that the SIL has a higher oxidative stability than the conventional electrolyte and, furthermore, offers the advantage of lower volatility, which would benefit an open-type lithium-O2 cell design. Moreover, CO2 evolution during galvanostatic charge was less in the SIL, which implies less side reaction. However, O2 evolution during charge did not reach the theoretical value in either of the two electrolytes. Several mass spectral fragments were generated during the charge process, which provided evidence for side reactions of glyme-based electrolytes. We further relate the difference in observed discharge product morphology for these electrolytes to the solubility of the superoxide intermediate, determined by rotating ring disk electrode (RRDE) measurements.

HTLV-1 bZIP factor suppresses apoptosis by attenuating the function of FoxO3a and altering its localization.

As the infectious agent causing human adult T-cell leukemia (ATL), the human T-cell leukemia virus type 1 (HTLV-1) virus spreads in vivo primarily by cell-to-cell transmission. However, the factors that determine its transmission efficiency are not fully understood. The viral genome encodes the HTLV-1 bZIP factor (HBZ), which is expressed in all ATL cases and is known to promote T-cell proliferation. In this study, we investigated the hypothesis that HBZ also influences the survival of T cells. Through analyzing the transcriptional profile of HBZ-expressing cells, we learned that HBZ suppressed transcription of the proapoptotic gene Bim (Bcl2l11) and that HBZ-expressing cells were resistant to activation-induced apoptosis. Mechanistic investigations into how HBZ suppresses Bim expression revealed that HBZ perturbs the localization and function of FoxO3a, a critical transcriptional activator of the genes encoding Bim and also Fas ligand (FasL). By interacting with FoxO3a, HBZ not only attenuated DNA binding by FoxO3a but also sequestered the inactive form of FoxO3a in the nucleus. In a similar manner, HBZ also inhibited FasL transcription induced by T-cell activation. Further study of ATL cells identified other Bim perturbations by HBZ, including at the level of epigenetic alteration, histone modification in the promoter region of the Bim gene. Collectively, our results indicated that HBZ impairs transcription of the Bim and FasL genes by disrupting FoxO3a function, broadening understanding of how HBZ acts to promote proliferation of HTLV-1-infected T cells by blocking their apoptosis.

Identification of physiological and toxic conformations in Abeta42 aggregates.

Aggregation of the 42-residue amyloid beta-protein (Abeta42) plays a crucial role in the pathogenesis of Alzheimer's disease (AD). Despite numerous structural studies on Abeta aggregates, the relationship between tertiary structure and toxicity remains unclear. Our proline scanning and solid-state NMR studies suggested that aggregates both of wild-type Abeta42 and of E22K-Abeta42 (one of the mutants related to cerebral amyloid angiopathy) contain two conformers: a major one with a turn at positions 25 and 26, and a minor one with a turn at positions 22 and 23. To identify the toxic conformer, the derivative Abeta42-lactam(22K-23E), in which the side chains at positions 22 and 23 were covalently linked, was synthesized as a minor conformer surrogate, along with Abeta42-lactam(25K-26E) as a major conformer surrogate. The Abeta42-lactam(22K-23E) showed stronger aggregation, neurotoxicity, radical generation, and oligomerization than wild-type Abeta42, whereas in Abeta42-lactam(25K-26E) were weak. The transition from the physiological conformation with a turn at positions 25 and 26 to the toxic conformation with a turn at positions 22 and 23 might be a key event in the pathogenesis of AD.

Verification of the intermolecular parallel beta-sheet in E22K-Abeta42 aggregates by solid-state NMR using rotational resonance: implications for the supramolecular arrangement of the toxic conformer of Abeta42.

Formation of the intermolecular beta-sheet is a key event in the aggregation of 42-residue amyloid-beta (Abeta42). We have recently identified a physiological and toxic conformer, the turn positions of which are slightly different from each other, in the aggregates of E22K-Abeta42 (one of the mutants related to cerebral amyloid angiopathy). However, it remains unclear whether the intermolecular beta-sheet in the E22K-Abeta42 aggregates is parallel or antiparallel. We prepared an equal mixture of E22K-Abeta42 aggregates labeled at C(alpha) and those labeled at C=O with (13)C, whose intermolecular (13)C-(13)C distance was estimated by solid-state NMR using rotational resonance (R2). The intermolecular proximity of beta-strands at positions 21 and 30 was less than 6 A, supporting the existence of the intermolecular parallel beta-sheet in the E22K-Abeta42 aggregates as well as in wild-type Abeta42 aggregates. The results also suggest that each conformer would not accumulate alternately, but form a relatively large assembly.

Verification of the C-terminal intramolecular beta-sheet in Abeta42 aggregates using solid-state NMR: implications for potent neurotoxicity through the formation of radicals.

Structural analysis of 42-residue amyloid beta (Abeta42) aggregates using rotational resonance in solid-state NMR verified that C(beta) and/or C(gamma) of Met-35 and the carboxyl carbon of Ala-42 are proximal enough to form an intramolecular antiparallel beta-sheet in the C-terminus. The S-oxidized radical cation at Met-35, an ultimate radical species responsible for neurotoxicity, could be stabilized by the carboxylate anion at the C-terminus, resulting in aggregation to cause long-term oxidative stress.